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Drug-Induced Death Signaling Strategy Rapidly Predicts Cancer Response to Chemotherapy

机译:药物诱导的死亡信号传导策略可快速预测癌症对化学疗法的反应

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摘要

There is a lack of effective predictive biomarkers to precisely assign optimal therapy to cancer patients. While most efforts are directed at inferring drug response phenotype based on genotype, there is very focused and useful phenotypic information to be gained from directly perturbing the patient's living cancer cell with the drug(s) in question. To satisfy this unmet need, we developed the Dynamic BH3 Profiling technique to measure early changes in net pro-apoptotic signaling at the mitochondrion ("priming") induced by chemotherapeutic agents in cancer cells, not requiring prolonged ex vivo culture. We find in cell line and clinical experiments that early druginduced death signaling measured by Dynamic BH3 Profiling predicts chemotherapy response across many cancer types and many agents, including combinations of chemotherapies. We propose that Dynamic BH3 Profiling can be used as a broadly applicable predictive biomarker to predict cytotoxic response of cancers to chennotherapeutics in vivo.
机译:缺乏有效的预测生物标记物,无法为癌症患者精确分配最佳治疗方法。尽管大多数努力都是基于基因型推断药物反应表型,但是通过直接用所研究的药物干扰患者的活癌细胞可以获得非常集中和有用的表型信息。为了满足这一未满足的需求,我们开发了动态BH3分析技术来测量癌细胞中化学治疗剂诱导的线粒体净促凋亡信号(“启动”)的早期变化,不需要长时间的离体培养。我们在细胞系和临床实验中发现,通过动态BH3分析测量的早期药物诱导的死亡信号传导可预测多种癌症类型和多种药物(包括化疗组合)的化疗反应。我们建议动态BH3分析可以用作广泛适用的预测性生物标志物,以预测体内癌症对鼻咽癌的细胞毒性反应。

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